Odiparcil, a potential glycosaminoglycans clearance therapy in mucopolysaccharidosis VI—Evidence from  in vitro  and  in vivo  models

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Abstract

Mucopolysaccharidoses are a class of lysosomal storage diseases, characterized by enzymatic deficiency in the degradation of specific glycosaminoglycans (GAG). Pathological accumulation of excess GAG leads to multiple clinical symptoms with systemic character, most severely affecting bones, muscles and connective tissues. Current therapies include periodic intravenous infusion of supplementary recombinant enzyme (Enzyme Replacement Therapy–ERT) or bone marrow transplantation. However, ERT has limited efficacy due to poor penetration in some organs and tissues. Here, we investigated the potential of the β-D-xyloside derivative odiparcil as an oral GAG clearance therapy for Maroteaux–Lamy syndrome (Mucopolysaccharidosis type VI, MPS VI). In vitro, in bovine aortic endothelial cells, odiparcil stimulated the secretion of sulphated GAG into culture media, mainly of chondroitin sulphate (CS) /dermatan sulphate (DS) type. Efficacy of odiparcil in reducing intracellular GAG content was investigated in skin fibroblasts from MPS VI patients where odiparcil was shown to reduce efficiently the accumulation of intracellular CS with an EC ₅₀ in the range of 1 μM. In vivo, in wild type rats, after oral administrations, odiparcil was well distributed, achieving μM concentrations in MPS VI disease-relevant tissues and organs (bone, cartilage, heart and cornea). In MPS VI Arylsulphatase B deficient mice ( Arsb ^-), after chronic oral administration, odiparcil consistently stimulated the urinary excretion of sulphated GAG throughout the treatment period and significantly reduced tissue GAG accumulation in liver and kidney. Furthermore, odiparcil diminished the pathological cartilage thickening observed in trachea and femoral growth plates of MPS VI mice. The therapeutic efficacy of odiparcil was similar in models of early (treatment starting in juvenile, 4 weeks old mice) or established disease (treatment starting in adult, 3 months old mice). Our data demonstrate that odiparcil effectively diverts the synthesis of cellular glycosaminoglycans into secreted soluble species and this effect can be used for reducing cellular and tissue GAG accumulation in MPS VI models. Therefore, our data reveal the potential of odiparcil as an oral GAG clearance therapy for MPS VI patients.

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Most cited references 64

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Biosynthesis and function of chondroitin sulfate.

Tadahisa Mikami, Hiroshi Kitagawa (2013)

Chondroitin sulfate proteoglycans (CSPGs) are principal pericellular and extracellular components that form regulatory milieu involving numerous biological and pathophysiological phenomena. Diverse functions of CSPGs can be mainly attributed to structural variability of their polysaccharide moieties, chondroitin sulfate glycosaminoglycans (CS-GAG). Comprehensive understanding of the regulatory mechanisms for CS biosynthesis and its catabolic processes is required in order to understand those functions.

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Golgi glycosylation.

Pamela Stanley (2011)

Glycosylation is a very common modification of protein and lipid, and most glycosylation reactions occur in the Golgi. Although the transfer of initial sugar(s) to glycoproteins or glycolipids occurs in the ER or on the ER membrane, the subsequent addition of the many different sugars that make up a mature glycan is accomplished in the Golgi. Golgi membranes are studded with glycosyltransferases, glycosidases, and nucleotide sugar transporters arrayed in a generally ordered manner from the cis-Golgi to the trans-Golgi network (TGN), such that each activity is able to act on specific substrate(s) generated earlier in the pathway. The spectrum of glycosyltransferases and other activities that effect glycosylation may vary with cell type, and thus the final complement of glycans on glycoconjugates is variable. In addition, glycan synthesis is affected by Golgi pH, the integrity of Golgi peripheral membrane proteins, growth factor signaling, Golgi membrane dynamics, and cellular stress. Knowledge of Golgi glycosylation has fostered the development of assays to identify mechanisms of intracellular vesicular trafficking and facilitated glycosylation engineering of recombinant glycoproteins.

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Cardiac disease in patients with mucopolysaccharidosis: presentation, diagnosis and management

Elizabeth A. Braunlin, Paul Harmatz, Maurizio Scarpa … (2011)

The mucopolysaccharidoses (MPSs) are inherited lysosomal storage disorders caused by the absence of functional enzymes that contribute to the degradation of glycosaminoglycans (GAGs). The progressive systemic deposition of GAGs results in multi-organ system dysfunction that varies with the particular GAG deposited and the specific enzyme mutation(s) present. Cardiac involvement has been reported in all MPS syndromes and is a common and early feature, particularly for those with MPS I, II, and VI. Cardiac valve thickening, dysfunction (more severe for left-sided than for right-sided valves), and hypertrophy are commonly present; conduction abnormalities, coronary artery and other vascular involvement may also occur. Cardiac disease emerges silently and contributes significantly to early mortality. The clinical examination of individuals with MPS is often difficult due to physical and, sometimes, intellectual patient limitations. The absence of precordial murmurs does not exclude the presence of cardiac disease. Echocardiography and electrocardiography are key diagnostic techniques for evaluation of valves, ventricular dimensions and function, which are recommended on a regular basis. The optimal technique for evaluation of coronary artery involvement remains unsettled. Standard medical and surgical techniques can be modified for MPS patients, and systemic therapies such as hematopoietic stem cell transplantation and enzyme replacement therapy (ERT) may alter overall disease progression with regression of ventricular hypertrophy and maintenance of ventricular function. Cardiac valve disease is usually unresponsive or, at best, stabilized, although ERT within the first few months of life may prevent valve involvement, a fact that emphasizes the importance of early diagnosis and treatment in MPS.

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Author and article information

Contributors

Eugeni Entchev:

ORCID: http://orcid.org/0000-0003-0744-5929

Role: ConceptualizationRole: InvestigationRole: MethodologyRole: SupervisionRole: Writing – original draftRole: Writing – review & editing

Ingrid Jantzen:

ORCID: http://orcid.org/0000-0001-6057-0724

Role: InvestigationRole: Methodology

Philippe Masson: Role: ConceptualizationRole: InvestigationRole: MethodologyRole: Supervision

Stephanie Bocart: Role: InvestigationRole: Methodology

Bruno Bournique: Role: InvestigationRole: Methodology

Jean-Michel Luccarini: Role: MethodologyRole: Project administrationRole: Supervision

Andre Bouchot: Role: InvestigationRole: Methodology

Olivier Lacombe: Role: MethodologyRole: Supervision

Jean-Louis Junien: Role: ConceptualizationRole: SupervisionRole: Writing – review & editing

Pierre Broqua: Role: ConceptualizationRole: SupervisionRole: Writing – review & editing

Mireille Tallandier: Role: ConceptualizationRole: Project administrationRole: SupervisionRole: Writing – review & editing

Sylvie Fournel-Gigleux: Role: Editor

Journal

Journal ID (nlm-ta): PLoS One

Journal ID (iso-abbrev): PLoS ONE

Journal ID (publisher-id): plos

Journal ID (pmc): plosone

Title: PLoS ONE

Publisher: Public Library of Science (San Francisco, CA USA )

ISSN (Electronic): 1932-6203

Publication date (Electronic): 15 May 2020

Publication date Collection: 2020

Volume: 15

Issue: 5

Electronic Location Identifier: e0233032

Affiliations

[1 ] Inventiva Pharma, Bourgogne-Franche-Comté, Daix, France

[2 ] DImaCell Core Facility, Inserm UMR1231 CellImaP site, Université de Bourgogne, Bourgogne-Franche-Comté, Dijon, France

UMR 7365 CNRS UL, FRANCE

Author notes

Competing Interests: I have read the journal’s policy and the authors of this manuscript have financial competing interests: PB is a co-founder and CSO of Inventiva; EE, IJ, OL, and MT are employees of Inventiva; JLJ is the Chairman of the Scientific Advisory Board and consultant for Inventiva and receives financial compensation from Inventiva; PM, SB, BB and JML were employees of Inventiva while the study was conducted; PM and JLJ are co-inventors on a patent for the use of odiparcil in the treatment of Mucopolysaccharidosis (FR1359657A); Inventiva affiliated authors (EE, IJ, PM, SB, BB, JML, OL, JLJ, PB and MT) have received stocks and shares from Inventiva; Odiparcil is being developed as a product for treatment of Mucopolysaccharidosis by Inventiva. AB is an employee of a company (DimaCell) that provided services on behalf of Inventiva. The authors confirm that “These do not alter our adherence to PLOS ONE policies on sharing data and materials”.

* E-mail: eugeni.entchev@ 123456inventivapharma.com (EE); mireille.tallandier@ 123456inventivapharma.com (MT)

Author information

Eugeni Entchev http://orcid.org/0000-0003-0744-5929

Ingrid Jantzen http://orcid.org/0000-0001-6057-0724

Article

Publisher ID: PONE-D-19-30400

DOI: 10.1371/journal.pone.0233032

PMC ID: 7228089

PubMed ID: 32413051

SO-VID: 5f2541d9-eee6-4726-9a2c-2c943daf471d

License:

This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

History

Date received : 31 October 2019

Date accepted : 27 April 2020

Page count

Figures: 8, Tables: 1, Pages: 22

Funding

This study is funded by Inventiva SA ("Inventiva"). Inventiva provided support in the form of salaries and other remuneration for authors (EE, IJ, PM, SB, BB, JML, OL, JLJ, PB and MT; see declared competing interests), but did not have any additional role in the study design, data collection and analysis, decision to publish, or preparation of the manuscript. The specific roles of these authors are articulated in the ‘author contributions’ section.

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Odiparcil, a potential glycosaminoglycans clearance therapy in mucopolysaccharidosis VI—Evidence from in vitro and in vivo models

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Most cited references 64

Biosynthesis and function of chondroitin sulfate.

Golgi glycosylation.

Cardiac disease in patients with mucopolysaccharidosis: presentation, diagnosis and management

Author and article information

Contributors

Journal

Affiliations

Author notes

Author information

Article

History

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Funding

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Comments

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Cited by 6

Most referenced authors 750